Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. I. Polyreactivity Could be Caused by Differential Glycosylation of Immunoglobulins

Fernández, Carmen; Alarcón-Riquelme, ME; Abedi‐Valugerdi, Manuchehr; Sverremark, Eva; Côrtes, Valdson de Angelis

doi:10.1046/j.1365-3083.1997.d01-397.x

Cited by 10 publications

(22 citation statements)

References 41 publications

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“…Binding to TNP was not influenced by Tm treatment while binding to other antigens was considerably reduced (Table 4 and Fig. 4) which is in accordance with our data in non-transgenic animals [6]. It is important to point out that differences in the stability of glycosylated and naked Igs and other trivial explanations can be excluded.…”

Section: The Influence Of Tm Treatment In Antigen Binding Of Transgensupporting

confidence: 90%

“…Per cent binding reduction was calculated by comparing equivalent points in the loglinear region of the binding curves. All these procedures have been described in detail elsewhere [6].…”

Section: Pcr (Polymerase Chain Reaction) Amplification and Sequencingmentioning

confidence: 99%

“…To assess the contribution of glycosylation in binding, we treated mono-and TNP/Dx/BSA-crossreactive clones with the inhibitor of glycosylation Tm [18,19,6]. Binding to TNP was not influenced by Tm treatment while binding to other antigens was considerably reduced (Table 4 and Fig.…”

Section: The Influence Of Tm Treatment In Antigen Binding Of Transgenmentioning

confidence: 99%

“…Per cent binding reduction was calculated by comparing equivalent points in the loglinear region of the binding curves. All these procedures have been described in detail elsewhere [6].Quantification of carbohydrate (CHO) content of lgs. The CHO content of polyreactive and monospecific MoAbs was evaluated by the digoxigenin (DIG) glycan-based method using a kit purchased from Boehringer Mannheim.…”

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Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. II. Crossreactive and Monospecific Antibodies can be Generated from an Identical Ig Rearrangement by Differential Glycosylation

1997

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Fernández C, Alarcón-Riquelme ME, Sverremark E. Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. II. Crossreactive and Monospecific Antibodies can be Generated from an Identical Ig Rearrangement by Differential Glycosylation. Scand J Immunol 1997;45:240-247 In this work the authors tested the hypothesis that differential glycosylation may be one of the mechanisms by which B cells could be able to produce monospecific or polyreactive antibodies flexibly. The same genetic information will be used in both situations. To prove this hypothesis the authors used mice transgenic for the SP6 (m þ k) hybridoma cell line producing monoclonal antibodies (MoAbs) with specificity for the hapten 2,4,6-trinitrophenyl (TNP). In these animals most cells in the periphery express exclusively the transgene SP6. To obtain polyreactive antibodies (Abs) spleen cells from transgenic animals were stimulated in vitro with lipopolysaccharide (LPS). The authors used LPS derived B cell blasts to produce a hybridoma cell collection. A high proportion of the monoclonal antibodies were found to bind to TNP and to crossreact with unrelated antigens. Endogenous immunoglobulins (lgs) were not responsible for crossreactivity since the crossreactive clones only expressed the transgene products. This was demonstrated by polymerase chain reaction (PCR) amplification of cDNA and by sequencing analysis of the PCR products. The nucleotide sequences of the expressed mono-and crossreactive genes were identical to the sequences of the rearranged V H and V K SP6 which undoubtedly demonstrates that crossreactive Igs are derived from the same rearrangement and also that no mutations in the V H or V K or in the CDR3 could account for the observed crossreactivity. It is also shown here that the crossreactive antibodies bear the idiotype Id 20-5 characteristic of SP6 binding Abs. Crossreactive monoclonal antibodies were found to be slightly more glycosylated than the TNP-monospecific Abs. Furthermore, binding to TNP was not influenced by treatment with tunicamycin, an inhibitor of glycosylation, while, in the same molecule, other types of binding were considerably reduced. This supports the hypothesis of the importance of glycosylation in polyreactivity. INTRODUCTIONIt is estimated that 30-80% of non-selected natural antibodies (Abs) are polyreactive [1][2][3][4]. A high level of polyreactivity is found after polyclonal B cell activation with lipopolysaccharide (LPS) [2,3,5]. It is uncertain whether the polyreactive Abs induced after LPS stimulation are different from the Abs in the specific pool or if the polyreactive Abs are modified specific Abs.In the accompanying article [6], we have shown elsewhere that 2-4% of the monoclonal antibodies (MoAbs) originated after stimulation with LPS bound to the carbohydrate dextran B512 (Dx), and that the vast majority of them were crossreactive with the unrelated antigen bovine serum albumin (BSA). We also demonstrated that crossreactive Abs were more sensitive to deglycosylation promoted b...

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Section: The Influence Of Tm Treatment In Antigen Binding Of Transgensupporting

confidence: 90%

“…Per cent binding reduction was calculated by comparing equivalent points in the loglinear region of the binding curves. All these procedures have been described in detail elsewhere [6].…”

Section: Pcr (Polymerase Chain Reaction) Amplification and Sequencingmentioning

confidence: 99%

Section: The Influence Of Tm Treatment In Antigen Binding Of Transgenmentioning

confidence: 99%

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confidence: 99%

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Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. II. Crossreactive and Monospecific Antibodies can be Generated from an Identical Ig Rearrangement by Differential Glycosylation

1997

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“…Binding to elements in the site might be related to the polyreactive behavior observed for immunoglobulins expressed by FL cells, 54 which, for antibody molecules, apparently can be influenced by glycosylation. 55,56 However, polyreactivity cannot be the only explanation because some myeloma proteins also exhibit this characteristic. 57 The location of the oligosaccharide in the V-region appears critical, possibly because, in contrast to the oligosaccharides in the constant region, 14 the chains exposed in the V-region may be more available to the glycosyl transferases and therefore may be fully glycosylated.…”

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Acquisition of potential N-glycosylation sites in the immunoglobulin variable region by somatic mutation is a distinctive feature of follicular lymphoma

Zhu

McCarthy

Ottensmeier

et al. 2002

Blood

243

204

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Further understanding of the nature of the cell of origin in FL has been provided by analysis of the immunoglobulin variableregion gene sequences of the tumor cells. During differentiation, normal B lymphocytes undergo a series of recombinatorial and mutational changes in their immunoglobulin variable-region genes. The V(D)J rearrangements of V H and V L genes occur mainly in the bone marrow, and, after encounter with antigen, the somatic mutation mechanism is activated in centroblasts in the GC. [1][2][3] In this site, certain mutated sequences are selected by antigens held on follicular dendritic cells, leading to affinity maturation of the antibody response. Survival, maturation, and subsequent fate of selected B cells are directed by several additional elements in the GC, including CD40L ϩ T cells and cytokine milieu. [1][2][3] For FL, it is clear that the cell of origin has undergone somatic mutation and that in many patients this process has continued after transformation, leading to intraclonal variation of V gene sequences. [4][5][6] This behavior is consistent with location in the GC. Because normal B cells rely on engagement of the B-cell receptor for activation of the mutation mechanism, the finding of continuing mutational activity has led to debate about the role of antigens in stimulating FL. 7 However, it appears that ongoing mutational activity may be limited in FL, 8 but it is not apparent in cases that have transformed to diffuse lymphoma after chemotherapy. 5,9 Uncertainty about the role of antigen in FL also cannot easily be resolved by analysis of mutational patterns in V genes because it is now evident that there is a natural tendency of the complementaritydetermining region (CDR) sequences to accumulate replacement mutations. 10 It remains unclear, therefore, whether antigen has a role in influencing the behavior of tumor cells in FL.However, the importance of immunoglobulin expression in FL is highlighted by the fact that in most patients with FL, expression is retained, in spite of the fact that one allele of chromosome 14 is commonly disrupted at 14q32 by the t(14;18) translocation. 11,12 Consequent overexpression of bcl-2 protein by the nonfunctional immunoglobulin allele is one mechanism that contributes to tumor cell survival. The almost universal conservation of immunoglobulin expression by the remaining functional allele might indicate a selective advantage for tumor cells in FL. The question arises as to whether this is dependent on stimulation by antigen.Immunoglobulin carries N-glycosylated oligosaccharides located mainly in the heavy-chain constant regions. These act as spacers for the immunoglobulin molecule that are important for For personal use only. on May 11, 2018. by guest www.bloodjournal.org From maintaining effector functions. 13 Because of locations of the sites in the interstitial region between the C H 2 domains, the oligosaccharide chains are incompletely galactosylated and sialylated. 14 Human antibodies do not generally contain O-linked oligosaccharides, wi...

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Mucosal Immunoglobulins

Woof

2015

Mucosal Immunology

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Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. I. Polyreactivity Could be Caused by Differential Glycosylation of Immunoglobulins

Cited by 10 publications

References 41 publications

Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. II. Crossreactive and Monospecific Antibodies can be Generated from an Identical Ig Rearrangement by Differential Glycosylation

Polyreactive Binding of Antibodies Generated by Polyclonal B Cell Activation. II. Crossreactive and Monospecific Antibodies can be Generated from an Identical Ig Rearrangement by Differential Glycosylation

Acquisition of potential N-glycosylation sites in the immunoglobulin variable region by somatic mutation is a distinctive feature of follicular lymphoma

Mucosal Immunoglobulins

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